Inactivation of nuclear Wnt-β-catenin signaling limits blastocyst competency for implantation

Citations Over TimeTop 10% of 2008 papers

Abstract

The activation of the blastocyst, a process by which it gains competency to attach with the receptive uterus, is a prerequisite for successful implantation. However, the molecular basis of blastocyst activation remains largely unexplored. Combining molecular, pharmacological and physiological approaches, we show here that silencing of Wnt-beta-catenin signaling in mice does not adversely affect the development of preimplantation embryos to blastocysts and uterine preparation for receptivity, but, remarkably, blocks blastocyst competency to implantation. Using the physiologically relevant delayed implantation model and trophoblast stem cells in culture, we further demonstrate that a coordinated activation of canonical Wnt-beta-catenin signaling with attenuation of the non-canonical Wnt-RhoA signaling pathway ensures blastocyst competency to implantation. These findings constitute novel evidence that Wnt signaling is at least one pathway that determines blastocyst competency for implantation.

Related Papers

• → Blastocysts don't go it alone. Extrinsic signals fine-tune the intrinsic developmental program of trophoblast cells(2005)124 cited
• → The Efficient Derivation of Trophoblast Cells from Porcine In Vitro Fertilized and Parthenogenetic Blastocysts and Culture with ROCK Inhibitor Y-27632(2015)32 cited
• → Comparative ultrastructure of hatched human, mouse and bovine blastocysts(1982)84 cited
• → THE MORPHOLOGY OF BLASTOCYST IMPLANTATION(1974)78 cited
• → The dynamic structure of rabbit blastocyst coverings(1988)24 cited